Background

Brain metastases are common in patients with melanoma, and optimal management is not well defined. As melanoma has traditionally been thought of as “radioresistant,” the role of whole brain radiation therapy (WBRT) in particular is unclear. We conducted this retrospective study to identify prognostic factors for patients treated with stereotactic radiosurgery (SRS) for melanoma brain metastases and to investigate the role of additional up-front treatment with whole brain radiation therapy (WBRT).

Methods

We reviewed records of 147 patients who received SRS as part of initial management of their melanoma brain metastases from January 2000 through June 2010. Overall survival (OS) and time to distant intracranial progression were calculated using the Kaplan-Meier method. Prognostic factors were evaluated using the Cox proportional hazards model.

Conclusions

Multiple brain metastases and omission of up-front WBRT (particularly in combination) are associated with distant intracranial progression. Improvement in intracranial disease control may be especially important in the subset of patients with absent or stable extracranial disease, where the competing risk of death from extracranial disease is low. These results are hypothesis generating and require confirmation from ongoing randomized trials.

Metastatic tumors from primary sites outside the central nervous system (CNS) are the most frequent intracranial neoplasms. Melanoma is among the primary tumors with the highest propensity for metastasis to the brain[1]. Up to half of patients with melanoma develop brain metastases, and once brain metastases are diagnosed, median survival time is estimated to range between 3.4 and 13.2 months[2, 3]. For individual patients, survival depends on a number of factors, and there has been much effort, both with brain metastases in general and with melanoma brain metastases specifically, to identify the factors that prognosticate for overall survival (OS)[4–11]. This information can be useful for patients and for their physicians who base treatment decisions in part on prognostic factor data.

Treatment options for patients with melanoma brain metastases include whole brain radiation therapy (WBRT), surgery, stereotactic radiosurgery (SRS), systemic therapy, some combination of these treatments, and supportive measures alone[3, 12]. SRS has become increasingly common, even for patients with multiple brain metastases[13–22], but some authors caution against the regular omission of up-front WBRT[20, 22]. Randomized data support adding WBRT to SRS for initial management of patients with brain metastases (not specific to patients with melanoma as the primary cancer) for the improvement of intracranial disease control, but not overall survival[23–25]. The translation of intracranial disease control to overall survival depends on competing risks from extracranial disease as well as the availability and efficacy of salvage options, suggesting that the impact of WBRT may differ depending on these factors. Data from a randomized trial of SRS alone versus SRS and WBRT specifically in patients with melanoma is not yet available[26], and retrospective studies are vulnerable to selection bias[13–18, 27].

In this retrospective study of melanoma patients treated with SRS for brain metastases, we sought to evaluate the potential utility of WBRT, given the lack of randomized evidence specific to this subpopulation, and to identify prognostic factors associated with OS and distant intracranial progression. Though we cannot eliminate selection bias altogether in a retrospective study examining the utility of WBRT, we sought to mitigate the effects of unmeasured confounders by leveraging inter-institutional practice variation.

Patient population

This study was approved by the Dana-Farber/Harvard Cancer Center Institutional Review Board.

We identified 243 consecutive patients with a histological diagnosis of melanoma who were treated with SRS for brain metastases from January 2000 through June 2010 at the Dana-Farber/Brigham & Women’s Cancer Center (DF/BWCC) or the Beth Israel Deaconess Medical Center (BIDMC). One patient was excluded due to lack of follow-up data. Thirty-five patients in whom SRS was performed only on a surgical resection cavity were also excluded. An additional 65 patients were excluded because SRS was performed only as salvage therapy. As a priori intention-to-treat could not be assigned retrospectively, salvage SRS was defined as any SRS performed greater than 3 months from the date of first treatment for brain metastases (i.e. the date of WBRT or surgery when these treatments were used prior to SRS) or any SRS performed for progression of intracranial disease (even if within 3 months of the first treatment). We reviewed records of the remaining 147 patients who received SRS as the initial management of their melanoma brain metastases. The follow-up schedule was not uniform in all cases, but the typical approach was to obtain brain magnetic resonance imaging (MRI) 6–8 weeks after SRS alone followed by MRI every 3 months thereafter if stable and every three months after WBRT.

Stereotactic radiosurgical technique

At DF/BWCC, SRS was performed using the Novalis™ linear accelerator-based radiosurgery platform. Prior to 2009, all patients were immobilized with the use of a fixed head frame. In 2009, conventional frame-based radiosurgery was replaced by frameless delivery using the thermoplastic BrainLAB cranial mask immobilization system. At BIDMC, SRS was performed using the X-Knife® linear accelerator-based radiosurgery platform or, beginning in 2005, the Cyberknife® platform.

Statistical analysis

Distant intracranial progression was defined as the presence of a new enhancing lesion consistent with a brain metastasis or leptomeningeal enhancement outside of the SRS target volume on any MRI after the date of SRS. Estimates of time to intracranial progression and OS were calculated using the Kaplan-Meier method. Time to distant intracranial progression was defined as the interval from SRS to the date of first distant intracranial progression (censored at the date of last MRI demonstrating no evidence of progression). OS was defined as the interval from SRS to the date of death (censored at the date of last clinical follow-up). The effects of clinical and demographic covariates on intracranial progression and OS were estimated using a Cox proportional hazards model. Variables with a p-value < 0.1 on univariate analysis were used to construct a multivariate model. (Age, as a continuous variable, was included in the multivariate model for OS regardless of significance on univariate analysis, given that for people in general, age is the most significant prognosticator for OS.) All other statistical tests used a significance level of 0.05 (two-sided) and a 95% confidence interval (95% CI). Analyses were performed using SAS (version 9.2) and R (version 3.0.3).

Clinical factors that were analyzed included patient age, Karnofsky Performance Status (KPS), number of brain metastases (one versus multiple), time from initial diagnosis of melanoma to SRS, use of up-front WBRT, the status of extracranial disease (absent or stable versus progressive), and the extent of extracranial metastases (limited versus extensive). In terms of extracranial disease status, “progressive” was defined as any evidence of new or progressing systemic disease on restaging computed tomography (CT) scan (by review of radiology reports and physician notes) within the 3 months prior to SRS. If no CT was available in the 3 months prior to SRS, then any restaging CT performed in the month following SRS was used. To define the extent of extracranial metastases, each patient was assigned a number between 0 and 6 based on evidence of any current (i.e. at the time of SRS) or past melanoma metastases to the following 6 sites: liver, lung, adrenal glands, other visceral organs, bone, or other distant site (e.g. lymph nodes or subcutaneous tissue). For example, if a particular patient had metastases to lungs, liver, and distant subcutaneous tissue, then the patient would be assigned a “3”. The median number of extracranial body sites affected by metastatic disease was used to dichotomize the extent-of-extracranial-metastases variable into “limited extracranial metastases” (less than or equal to the median number of body sites affected by metastatic melanoma) and “extensive extracranial metastases” (greater than the median number of body sites affected by metastatic melanoma).

Patient characteristics

The median follow-up time for survivors was 23 months. The frequency of clinical covariates is shown in Table 1. Median age was 60 years. Eighty patients (54%) had KPS of 90% or 100%; 61 patients (41%) had KPS of 70% or 80%; and 6 patients (4%) had KPS of 50% or 60%. Thirty-five patients (24%) had absent or stable extracranial metastases, while 112 patients (76%) had progressive extracranial disease. The median number of extracranial sites affected by metastatic melanoma was 2. Eighty-six patients (59%) had “limited extracranial metastases” (i.e. ≤ 2 sites affected by metastatic melanoma), and 61 patients (41%) had “extensive extracranial metastases” (i.e. ≥ 3 extracranial sites affected by metastatic melanoma) At DF/BWCC, 54% of patients were initially treated with WBRT in addition to SRS (i.e. “up-front WBRT”), while only 3% of patients had up-front WBRT at BIDMC. An additional 13% of patients at DF/BWCC and 30% of patients at BIDMC received salvage WBRT. Only 2 of 59 patients (3%) with one brain metastasis received up-front WBRT, while 37 of 88 patients (42%) with multiple brain metastases did so. The use of up-front WBRT was associated with treatment center (Fisher’s exact test: p < 0.0001) and multiple brain metastases (p < 0.0001). The median number of brain metastases for patients receiving WBRT up front was 4 (IQR 3–5) while those treated with SRS alone was 1 (IQR 1–2).

*To define the “extent of extracranial metastases”, each patient was assigned a number between 0 and 6 based on evidence of melanoma metastases to the following 6 sites: liver, lung, adrenal glands, other visceral organs, bone, or other distant site (e.g. lymph nodes or subcutaneous tissue). The median number of extracranial body sites affected by metastatic melanoma is 2. “Limited extracranial metastases” was defined as ≤ 2 extracranial body sites affected by metastatic melanoma. “Extensive extracranial metastases” was defined as ≥ 3 extracranial body sites affected by metastatic melanoma.

†Systemic Treatment with SRS = systemic treatment given after SRS and before disease progression.

Intracranial progression

Fifty-six patients had distant failure prior to any local failure (i.e. progression within the SRS treatment field); 20 had distant and local failure at the same time; and 27 people had local failure first (10 of these 27 people went on to develop distant intracranial progression at a later time). Therefore, distant intracranial progression occurred in a total of 86 patients (59%). Median time to distant intracranial progression was 4.3 months. Table 2 lists the results of Cox regression analysis for time to distant intracranial progression. On multivariate analysis, age > 60 years (hazard ratio [HR] 0.64, p = 0.05), multiple brain metastases (HR 1.90, p = 0.008), and omission of up-front WBRT (HR 2.24, p = 0.005) were associated with distant intracranial progression. In patients with multiple brain metastasis, median time to distant intracranial progression was 2.0 months in patients in whom WBRT was initially omitted (i.e. those treated with SRS alone or SRS and surgery as initial treatment), and 6.0 months in patients treated with up-front WBRT (in addition to up-front SRS [and, in some cases, up-front surgery as well]) (p = 0.003). In patients with a single brain metastasis, however, the median time to distant intracranial progression was approximately 5 months, both in patients treated with up-front WBRT and in patients in whom WBRT was initially omitted. Figure 1 shows the Kaplan-Meier curves for distant intracranial progression by use of up-front WBRT in the subset of 88 patients with multiple brain metastases. In terms of local failure (i.e. growth of the lesion[s] within the SRS treatment field), on Cox univariate analysis, both WBRT (HR 2.56, p = 0.02) and diameter of largest brain metastasis (diameter >1 cm: HR 2.70, p = 0.03) were associated with local failure first (i.e. local progression taking place prior to distant intracranial progression), but WBRT was not significant on multivariate analysis or when number of brain metastases was added to the model. Of the patients who did not receive up-front WBRT and who subsequently failed, 42% received WBRT as salvage therapy.

*Age (as a continuous variable) was included in multivariate models for overall survival regardless of significance on univariate analysis.

†See Materials and Methods section and Table 1 for definitions of extensive and limited extracranial metastases.

Subset analysis in patients with absent or stable extracranial disease

We repeated the Cox regression analyses in the subset of 35 patients with absent or stable extracranial disease. Multiple brain metastases (HR 4.64 [95% CI 1.54 – 13.94], p = 0.006) and omission of up-front WBRT (HR 3.14 [95% CI 1.02-9.68, p = 0.05) were associated with distant intracranial progression in the multivariate model. The final multivariate model for OS in this subset contained age (as a continous variable; HR 1.02, p = 0.24), multiple brain metastases (HR 5.89 [95% CI 1.79 – 19.43], p = 0.004), and omission of up-front WBRT (HR 2.56 [95% CI 0.91 – 7.23], p = 0.08). Therefore, there was a trend toward worse OS with omission of up-front WBRT. When any WBRT (including up-front and salvage WBRT) was put in the Cox model in place of the up-front-WBRT variable, there was no such trend. Figure 2 shows the Kaplan-Meier curves for OS by number of brain metastases in the subset of 35 patients with absent/stable extracranial disease (Figure 2B) and in the subset of 112 patients with progressive extracranial disease (Figure 2A). Given that extent of extracranial metastases (limited vs. extensive) – not the status of extracranial disease (absent/stable vs. progressive) – was associated with OS in the entire cohort, a subset analysis was also performed in patients with limited extracranial disease. When both number of brain metastases and up-front WBRT were entered into the Cox regression model for OS in the 86 patients with limited extracranial disease, there was a trend toward an association with worse OS for multiple brain metastases, but WBRT was not significant.

Figure 2

Kaplan-Meier curves for overall survival by number of brain metastases, separated by extracranial disease status. (A: Subset of patients with progressive extracranial disease. B: Subset of patients with absent or stable extracranial disease). (One patient with progressive extracranial disease in the multiple brain metastasis group was censored at 75 months, and one patient with absent/stable disease in the single brain metastasis group was censored at 102 months [not shown in figure]). (Logrank for 112 patients with progressive extracranial disease: p = 0.59. Logrank for 35 patients with absent/stable extracranial disease: p = 0.01). Abbreviations: SRS = stereotactic radiosurgery.

In our series of patients with melanoma brain metastases treated with SRS, multiple brain metastases and omission of up-front WBRT were associated with distant intracranial progression. Whether or not the factors associated with freedom from distant intracranial progression would also be expected to improve OS depends partly on the issue of competing risk, that is, whether intracranial disease or extracranial disease is the main driver of mortality. If mortality is driven by intracranial disease, then factors that improve intracranial disease control, such as fewer brain metastases and the initial use of WBRT with SRS, would also be expected to improve OS. On the other hand, if extracranial disease is driving mortality, then extracranial disease burden (e.g. the extent of extracranial metastases) and status (e.g. whether the extracranial disease is stable or progressing) would be expected to affect mortality, while number of brain metastases and WBRT would not. Indeed, in our study, none of the factors that improved freedom from distant intracranial progression (or freedom from local failure) was in our final model for OS. Extracranial disease, more so than intracranial disease factors or progression, appears to drive mortality in the overall cohort.

In our analysis of the subset of patients with absent or stable extracranial disease, the factors associated with improved survival were those related to intracranial disease. Specifically, of the three factors associated with distant intracranial progression in the entire cohort, one (i.e. multiple brain metastases) was also associated with poor OS in the subset analysis (p = 0.004), and another (i.e. omission of up-front WBRT) demonstrated a trend toward such an association (p = 0.08). Extracranial disease status may, therefore, modify the effect of intracranial disease burden (and control) on OS, such that the number of brain metastases (and the use of up-front WBRT) is prognostic for survival in patients with absent or stable extracranial metastases, but not in patients with progressive extracranial disease.

Recently we argued that for certain cancers, such as lung cancer, the presence versus absence of extracranial disease may be an appropriate surrogate for overall extracranial disease burden, whereas a more granular approach may be necessary for other cancers[28]. In our series of 51 patients treated with SRS for breast cancer brain metastases, extracranial disease status, measured as absent or stable versus progressive (as opposed to absent versus present), was our most robust prognostic factor for OS and added pertinent additional information to the established prognostic index, the Graded Prognostic Assessment (GPA)[28]. For patients with melanoma, where 92% and 76% of the patients in our cohort had present and progressive extracranial disease, respectively, an even more granular measure may be necessary. Indeed the “extent of extracranial metastases” variable that we defined for this study may better capture the overall burden of extracranial disease in patients with metastatic melanoma. Even this variable is an imperfect proxy for overall disease burden, however. Other groups have also shown the importance of extracranial disease as a prognostic factor for OS in patients with melanoma brain metastases, and some did so by measuring lactate dehydrogenase (LDH) level, which may also capture the extent of extracranial disease in a more granular fashion[9–11, 15, 17]. Adding some surrogate for extracranial disease burden to existing prognostic indices that do not already include such a factor may improve these indices.

The data regarding the use of WBRT for patients with melanoma are mixed, with some authors arguing that melanoma is a radioresistant tumor with limited benefit from non-SRS radiation treatments[14]. Some studies have shown no benefit of WBRT for melanoma brain metastases[13–15, 27, 29], while others suggest WBRT may improve intracranial disease control[17] or survival[18]. Several studies acknowledge that the absence of an observed effect of WBRT on intracranial disease control or survival might be due to selection bias. While we are not able to eliminate unmeasurable selection bias in this retrospective study, we hopefully diminished its effects with respect to WBRT by including patients from two treatment centers with different institutional practices. One center frequently performed both SRS and WBRT as part of initial management of melanoma brain metastases (particularly in those with more than one brain metastasis), while the other rarely did so. Even with this attempt to diminish selection bias in our study, the use of WBRT was as strongly associated with multiple brain metastases as it was with treatment center. Our results do, however, suggest that WBRT added to SRS improves freedom from distant intracranial progression (especially in patients with multiple brain metastases), providing some evidence that melanoma is not as uniformly radioresistant (and that the utility of WBRT in melanoma is not as limited) as some have argued. Whether the reduction in distant intracranial failure is clinically important in the overall course of the disease is in question, but the effect of WBRT in reducing failure is less so, given our data.

One limitation of our study is the degree to which we are able to address the question of whether improved intracranial control matters. Whether improvements in intracranial control translate to a more meaningful clinical benefit (such as overall survival) depends not only on competing risk, but also on the efficacy of salvage options. We could not directly compare up-front WBRT to salvage WBRT, as only 42% of eligible patients received salvage WBRT. Our data does not provide direct evidence to either support or refute any claim on this issue, but the trend toward better OS with the initial use of WBRT in patients with absent or stable extracranial disease may suggest imperfect salvage options. Furthermore, while our institutional practice has been to obtain surveillance MRI every 3 months, this could not be standardized in a retrospective study and the potential impacts of more frequent monitoring on salvage options and efficacy is unknown.

Multiple randomized trials of WBRT and SRS versus SRS alone in patients with brain metastases from various primary cancers (mostly lung and breast cancers) suggest that WBRT does not improve OS[23–25]. Yet in certain primary cancers, especially in those that are more likely to have progressive intracranial disease as a source of mortality, the improvements in intracranial control caused by WBRT may theoretically contribute to a survival benefit. Such cancers may act more aggressively in the CNS or have a more limited risk of extracranial disease progression. Whether melanoma fits into this category is currently unknown. Conversely, if extracranial disease progression is the primary driver of mortality, then WBRT may have a very limited role in addition to focal therapies, as prophylaxis against distant brain metastases may not be clinically relevant in such a scenario. Additionally, more frequent MRI surveillance may increase the efficacy of salvage therapy, obviating the need for upfront WBRT. A randomized, phase III trial of local therapy (neurosurgical resection and/or SRS) with or without WBRT for patients with melanoma brain metastases is currently being conducted by the Australia and New Zealand Melanoma Trials Group and the Trans Tasman Radiation Oncology Group[26]. In this trial, randomization is stratified by extracranial disease status. Such randomized trials that stratify by extracranial disease status may have the best potential for confirming our findings and the findings from other retrospective studies.

In summary, we identified multiple brain metastases and the omission of up-front WBRT (particularly in those with multiple brain metastases) as factors associated with distant intracranial progression after SRS. The effect of these factors on OS was modified by extracranial disease status, such that multiple brain metastases and (to a degree that could be characterized as a trend) omission of up-front WBRT were associated with worse OS in patients with absent or stable extracranial disease, but not in those with progressive extracranial disease. The data also confirm the significance of KPS for OS and suggest that extracranial disease burden (as measured by the number of extracranial body sites affected by melanoma metastases) may be an important factor for OS in the general population of patients undergoing SRS for melanoma brain metastases. As the ability to control systemic disease in patients with metastatic melanoma improves, the contribution of intracranial disease burden and control in helping to determine OS may increase.

Acknowledgments

This work was funded by a generous donation from Ronald Martin and Family. Ronald Martin and Family had no role in study design, data collection, data analysis, data interpretation, writing of the manuscript, or decision to submit the manuscript for publication.

Authors' original submitted files for images

Below are the links to the authors’ original submitted files for images.

Competing interests

Dr. Hodi reports non-paid consultancy and institute receipt of clinical trial support from Bristol-Myers Squibb, non-paid consultancy and institute receipt of clinical trial support from Merck, non-paid consultancy and institute receipt of clinical trial support from Genetech, personal fees from Amgen, and personal fees from Novartis. However, none of these companies or the relationships Dr. Hodi has with these companies will benefit or suffer from the publication of this manuscript.

Authors’ contributions

MAD participated in study design, data entry, data analysis, and writing of the manuscript. NDA, EQL, FSH, NI, SEW, and SRF helped with study design and drafting of the manuscript. YC carried out statistical analysis and participated in study design. NEP, TM, and PJK helped with data entry/database design, study design, and drafting of the manuscript. AM and BMA oversaw the study and participated in study design and writing of the manuscript. All authors read and approved the final manuscript.

This article is published under license to BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

By submitting a comment you agree to abide by our Terms and Community Guidelines. If you find something abusive or that does not comply with our terms or guidelines please flag it as inappropriate. Please note that comments may be removed without notice if they are flagged by another user or do not comply with our community guidelines.